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Co-operation between enhancers modulates quantitative expression from the Drosophila Paramyosin/miniparamyosin gene in different muscle types

机译:增强子之间的合作调节果蝇副肌球蛋白/小副肌球蛋白基因在不同类型肌肉中的定量表达

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摘要

The distinct muscles of an organism accumulate different quantities of structural proteins, but always maintaining their stoichiometry. However, the mechanisms that control the levels of these proteins and that co-ordinate muscle gene expression remain to be defined. The paramyosin/miniparamyosin gene encodes two thick filament proteins transcribed from two different promoters. We have analysed the regulatory regions that control expression of this gene and that are situated in the two promoters, the 5′ and the internal promoters, both in vivo and in silico. A distal muscle enhancer containing three conserved MEF2 motifs is essential to drive high levels of paramyosin expression in all the major embryonic, larval and adult muscles. This enhancer shares sequence motifs, as well as its structure and organisation, with at least four co-regulated muscle enhancers that direct similar patterns of expression. However, other elements located downstream of the enhancer are also required for correct gene expression. Other muscle genes with different patterns of expression, such as miniparamyosin, are regulated by other basic mechanisms. The expression of miniparamyosin is controlled by two enhancers, AB and TX, but a BF modulator is required to ensure the correct levels of expression in each particular muscle. We propose a mechanism of transcriptional regulation in which similar enhancers are responsible for the spatio-temporal expression of co-regulated genes. However, it is the interaction between enhancers which ensures that the correct amounts of protein are expressed at any particular time in a cell, adapting these levels to their specific needs. These mechanisms may not be exclusive to neural or muscle tissue and might represent a general mechanism for genes that are spatially and temporally co-regulated. © 2005 Elsevier Ireland Ltd. All rights reserved.
机译:生物体的不同肌肉积累不同数量的结构蛋白,但始终保持其化学计量。但是,控制这些蛋白质水平和协调肌肉基因表达的机制仍有待确定。副肌球蛋白/小副肌球蛋白基因编码从两个不同启动子转录的两个粗丝蛋白。我们已经分析了在体内和计算机模拟中控制该基因表达的调节区,该调节区位于两个启动子5'和内部启动子中。包含三个保守的MEF2基序的远端肌肉增强剂对于在所有主要的胚胎,幼虫和成年肌肉中驱动高水平的副肌球蛋白表达至关重要。该增强子与至少四个共同指导相似表达模式的肌肉增强子共享序列基序及其结构和组织。然而,正确基因表达也需要位于增强子下游的其他元件。其他表达方式不同的肌肉基因,例如小副肌球蛋白,受其他基本机制调控。 miniparamyosin的表达受两种增强剂AB和TX的控制,但是需要BF调节剂来确保每个特定肌肉中正确的表达水平。我们提出了一种转录调控机制,其中相似的增强子负责共同调控基因的时空表达。但是,增强剂之间的相互作用确保了在细胞中的任何特定时间表达正确数量的蛋白质,从而使这些水平适应其特定需求。这些机制可能并非神经或肌肉组织所独有,它们可能代表了在空间和时间上共同调控的基因的一般机制。 ©2005爱思唯尔爱尔兰有限公司。保留所有权利。

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